Literature DB >> 28163212

Exogenous vitamin C boosts the antitumor efficacy of paclitaxel containing reduction-sensitive shell-sheddable micelles in vivo.

Yaqin Zhu1, Xiuxiu Wang2, Jian Zhang2, Fenghua Meng2, Chao Deng2, Ru Cheng2, Jan Feijen3, Zhiyuan Zhong4.   

Abstract

Slow drug release at the tumor tissue and poor tumor penetration are two big challenges for the successful application of nanosystems in tumor therapy. Here, we report that a high concentration of the natural reducing agent vitamin C (VC) triggers rapid extracellular PTX release from PTX-loaded shell-sheddable PEG-SS-PCL micelles (SSM) in tumors in vivo. An in vivo tolerance study showed that VC at a blood concentration of 40mM had little toxicity to nude mice. Notably, SSM rapidly disassembled and released the payloads (Cy5 or PTX) in response to 40mM VC. In vivo near-infrared imaging of tumor-bearing mice showed that with post-injection of VC to establish a blood concentration of 40mM, Cy5 was quickly released from the micelles and diffused deep into the tumor tissue. Biodistribution studies revealed that 6h after the injection of PTX-loaded micelles the highest tumor accumulation was reached, which was set as the injection time for VC. The antitumor efficacy of a combination therapy of PTX-loaded micelles and VC was evaluated in both MCF-7 and U87MG tumor models. In both tumor models, single injections of VC didn't show any antitumor effect, while sequential administration of PTX-loaded SSM and VC exhibited significantly higher tumor inhibition effects and better survival rates as compared to single treatment with PTX-loaded micelles, demonstrating that exogenous administration of VC effectively triggered the release of PTX from SSM in vivo. The combination of reduction-sensitive nanomedicines with exogenous VC appears a promising approach to achieve potent treatment of malignant tumors.
Copyright © 2017 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  Biodegradable micelles; Drug release; Paclitaxel; Reduction-sensitive; Tumor penetration; Vitamin C

Mesh:

Substances:

Year:  2017        PMID: 28163212     DOI: 10.1016/j.jconrel.2017.02.002

Source DB:  PubMed          Journal:  J Control Release        ISSN: 0168-3659            Impact factor:   9.776


  6 in total

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Authors:  Di Chen; Xinyue Wei; Ke Yang; Xinyue Liu; Yujin Song; Futing Bai; Yi Jiang; Yuhang Guo; Rajiv Kumar Jha
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2.  Ascorbic acid induced TET2 enzyme activation enhances cancer immunotherapy efficacy in renal cell carcinoma.

Authors:  Ding Peng; Anbang He; Shiming He; Guangzhe Ge; Shuo Wang; Weimin Ci; Xuesong Li; Dan Xia; Liqun Zhou
Journal:  Int J Biol Sci       Date:  2022-01-01       Impact factor: 6.580

3.  Shell-Sheddable Micelles Based on Poly(ethylene glycol)-hydrazone-poly[R,S]-3-hydroxybutyrate Copolymer Loaded with 8-Hydroxyquinoline Glycoconjugates as a Dual Tumor-Targeting Drug Delivery System.

Authors:  Adrian Domiński; Monika Domińska; Magdalena Skonieczna; Gabriela Pastuch-Gawołek; Piotr Kurcok
Journal:  Pharmaceutics       Date:  2022-01-26       Impact factor: 6.321

4.  PEGylated self-assembled enzyme-responsive nanoparticles for effective targeted therapy against lung tumors.

Authors:  Fangyuan Guo; Jiangqing Wu; Wenchao Wu; Dongxue Huang; Qinying Yan; Qingliang Yang; Ying Gao; Gensheng Yang
Journal:  J Nanobiotechnology       Date:  2018-07-16       Impact factor: 10.435

5.  Oxidation- and Temperature-Responsive Poly(hydroxyethyl acrylate-co-phenyl vinyl sulfide) Micelle as a Potential Anticancer Drug Carrier.

Authors:  Tae Hoon Kim; Madhusudhan Alle; Jin-Chul Kim
Journal:  Pharmaceutics       Date:  2019-09-06       Impact factor: 6.321

6.  Poly(ethylene glycol)-sheddable reduction-sensitive polyurethane micelles for triggered intracellular drug delivery for osteosarcoma treatment.

Authors:  Zhengjie Yang; Qianping Guo; Yan Cai; Xuesong Zhu; Caihong Zhu; Yuling Li; Bin Li
Journal:  J Orthop Translat       Date:  2019-12-06       Impact factor: 5.191

  6 in total

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